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增强子功能的发育性获得需要独特的共激活因子活性。

Developmental acquisition of enhancer function requires a unique coactivator activity.

作者信息

Majumder S, Zhao Z, Kaneko K, DePamphilis M L

机构信息

University of Texas MD Anderson Cancer Center, Houston 77030, USA.

出版信息

EMBO J. 1997 Apr 1;16(7):1721-31. doi: 10.1093/emboj/16.7.1721.

Abstract

Enhancers are believed to stimulate promoters by relieving chromatin-mediated repression. However, injection of plasmid-encoded genes into mouse oocytes and embryos revealed that enhancers failed to stimulate promoters prior to formation of a two-cell embryo, even though the promoter was repressed in the maternal nucleus of both oocytes and one-cell embryos. The absence of enhancer function was not due to the absence of a required sequence-specific enhancer activation protein, because enhancer function was not elicited even when these proteins either were provided by an expression vector (GAL4:VP16) or were present as an endogenous transcription factor (TEF-1) and shown to be active in stimulating promoters. Instead, enhancer function in vivo required a unique coactivator activity in addition to enhancer-specific DNA binding proteins and promoter repression. This coactivator activity first appeared during mouse development in two- to four-cell embryos, concurrent with the major onset of zygotic gene expression. Competition between various enhancers was observed in these embryos, but not competition between enhancers and promoters, and competition between enhancers was absent in one-cell embryos. Moreover, enhancer function in oocytes could be partially restored by pre-injecting mRNA from cells in which enhancers were active, the same mRNA did not affect enhancer function in two- to four-cell embryos.

摘要

增强子被认为是通过解除染色质介导的抑制作用来刺激启动子。然而,将质粒编码基因注射到小鼠卵母细胞和胚胎中发现,在二细胞胚胎形成之前,增强子无法刺激启动子,尽管启动子在卵母细胞和单细胞胚胎的母细胞核中受到抑制。增强子功能的缺失并非由于缺少必需的序列特异性增强子激活蛋白,因为即使这些蛋白由表达载体(GAL4:VP16)提供或作为内源性转录因子(TEF-1)存在并被证明在刺激启动子方面具有活性,增强子功能也未被引发。相反,体内增强子功能除了需要增强子特异性DNA结合蛋白和启动子抑制外,还需要一种独特的共激活因子活性。这种共激活因子活性在小鼠发育过程中首次出现在二至四细胞胚胎中,与合子基因表达的主要起始同时发生。在这些胚胎中观察到了各种增强子之间的竞争,但没有观察到增强子与启动子之间的竞争,并且在单细胞胚胎中不存在增强子之间的竞争。此外,通过预先注射来自增强子活跃细胞的mRNA,可以部分恢复卵母细胞中的增强子功能,而相同的mRNA对二至四细胞胚胎中的增强子功能没有影响。

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